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1

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Primary malignant rhabdoid tumours of the central nervous system: An immunohistochemical and ultrastructural study (1997)

Bergmann, M. ; Spaar, H. J. ; Ebhard, G. ; [et al.]

Springer

Acta neurochirurgica 139 (1997), S. 961-969

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ISSN: 0942-0940

Keywords: Malignant rhabdoid tumour ; atypical teratoid/rhabdoid tumour

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Three cases of primary rhabdoid tumour of the CNS (RT-CNS) are presented. In case 1 a hemispheric tumour developed in a 10.5 months old girl, who survived for 6 months after incomplete resection, radio- and polychemotherapy. Case 2 was a 4 years and 8 months old boy with a large IIIrd ventricle tumour, who died of leptomeningeal tumour dissemination 7 months after diagnosis despite radiotherapy. In case 3 a pineal mass occurring in a 14 month old female was radioresistant and totally exstirpated. The child died due to tumour recurrence two months later. Autopsy examination revealed widespread leptomeningeal dissemination. All three cases fulfilled light and electron microscopic criteria of RT-CNS including abundant eosinophilic cytoplasm, vesicular nuclei with large nucleoli and conspicuous anti-vimentin positive filaments. Extensive immunohistochemical studies showed expression of epithelial (EMA, KL1), macrophage (alpha-1 antichymotrypsin), neuro-ectodermal (GFAP, NSE, β-tubulin III) and myogenic markers (desmin, actin). Different stress proteins (alpha-B crystallin, HSP70) were also expressed. Tumour cells showed a proliferation (MIB1) index of 28.4% (case 1) and 33.4% (case 2). From our study it can be concluded that RT-CNS reveals significant immuno-morphological heterogeneity thus supporting the view that it is not a specific pathological entity but merely a phenotypic appearance of different neoplasms, some of which are linked to primitive neuro-ectodermal tumours.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01411306

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2

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Response of detector modules of the neutron hodoscope SENECA to neutrons with energies 7-70 MeV

v. Edel, G. ; Selke, O. ; Poch, C. ; [et al.]

Amsterdam : Elsevier

Nuclear Instruments and Methods in Physics Research Section A: 332 (1993), S. 224-231

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ISSN: 0168-9002

Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002

Topics: Physics

Type of Medium: Electronic Resource

URL: http://linkinghub.elsevier.com/retrieve/pii/0168-9002(93)90763-8

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3

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Selection of liver-colonizing tumor cells from a murine fibrosarcoma induced by methylcholanthrene (1984)

Edel, G. ; Grundmann, E.

Springer

Journal of cancer research and clinical oncology 108 (1984), S. 274-280

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ISSN: 1432-1335

Keywords: Metastasis ; Organ preference of metastasis ; MCA-induced murine fibrosarcoma ; Tumor model

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary An experimental tumor model was developed to study the organ preference of malignant tumors. The primary tumor ER 15-P was induced by in-oculation of 1 mg methylcholanthrene in 0.1 ml sesame oil into the left femoral muscle of a female C57/B16J mouse. The tumor was palpable 100 days after induction. Spontaneous lung metastases were found at autopsy on day 128. Serial IM transplantation of tumor cells from the primary ER 15-P resulted in pulmonary metastases in all male and female mice. After IV injection of tumor cells from ER 15-P to male mice, colonies were found in lungs, thoracic cavity, liver, kidneys and occasionally also adrenals; female mice sometimes had ovarian metastases in addition, but no hepatic metastases. Liver-colonizing tumor cells were selected in male mice as follows: (a) IV injection of tumor cells from primary ER 15-P; (b) removal of tumor cells from liver tumor nodules, reinjection into mesenteric vein; (c) preparation of resulting tumors in the liver, reinjection of these cells through the portal system in one group of mice, and IV administration into tail vein in another group: (d) IM inoculation of tumor cells of the mesenteric passage in the left gastrocnemius muscle of mice prior to IV injection via tail vein in another group. Steps c and d were repeated three times. The procedure resulted in a highly significant decrease of tumor cell colonization to lungs and other organs, and a preferential increase of liver colonization. The liver preference of cell lines thus selected was obvious. Possible mechanisms for the organ preference of malignant tumors are discussed.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00390457

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4

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The influence of the microenvironment on liver-specific tumor cell colonization in a murine tumor model (1988)

Edel, G.

Springer

Journal of cancer research and clinical oncology 114 (1988), S. 163-169

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ISSN: 1432-1335

Keywords: Metastases ; Organ preference ; Microenvironment ; MCA-induced murine myofibrosarcoma ; Tumor model ER 15-P

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Malignant tumors often show an organ-specific metastatic spread. Some cells of the primary apparently bear an affinity for growing in the microenvironment of certain organs. After i.v. injection of myofibrosarcoma cells from the primary ER 15-P into the tail vein of male C57/BI6J mice, metastases developed in various organs. A tumor cell line (ER 15-Me3) isolated from liver metastases of the primary was found to colonize preferentially to the liver. To find out whether the liver specificity of the tumor cell line ER 15-Me3 depended on the hepatic microenvironment, tumor cells from this line were transplanted i.m. into the thighs of mice once (ER 15-Me3 i.m.1) or 5 times (ER 15-Me3 i.m.5), and then injected into the tail vein of mice. A part of the 5-times passaged tumor cell line was also injected into the mesenteric vein (ER 15-Me3 i.m.5-Me1) prior to reinjection into the tail vein. Results: After i.v. administration of tumor cells from the first i.m. passage of the tumor cell line (ER 15-Me3 i.m.1) into the tail vein, the liver-specific metastatic behavior of tumor cells remained stable. Following the i.v. injection of tumor cells from the 5th i.m. transplant generation of the tumor cell line (ER 15-Me3 i.m.5) into the tail vein, organ distribution was similar to that of the primary. After only 1 mesenteric vein passage of the 5-times i.m. transplanted line ER 15-Me3 i.m.5-Me1 followed by i.v. injection into the tail vein, did tumor cells regain their liver-specific colonizing potential. Thus, the liver-specific tumor cell line seems to contain a small number of other tumor cell populations from the unselected primary. In the muscle, these tumor cells have a growth advantage over the liver-specific cells, while the latter will grow better in the liver. This indicates that the microenvironment may be one important factor influencing the organ-specific metastatic pattern of tumor cells.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00417831

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5

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Morphological heterogeneity and phenotypical instability versus metastatic stability in the murine tumor model ER 15-P (1992)

Edel, G. ; Roessner, A. ; Deneke, B. ; [et al.]

Springer

Journal of cancer research and clinical oncology 118 (1992), S. 349-360

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ISSN: 1432-1335

Keywords: Pleomorphic myofibrosarcoma ER 15-P ; Morphological heterogeneity ; Lung metastases ; Metastatic potential

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary At clinical presentation, the majority of malignant tumors are composed of multiple clonal subpopulations of tumor cells with different phenotypic characteristics. Using the experimental tumor model ER 15-P, a methylcholanthrene-induced pleomorphic sarcoma of the C57 Bl6J mouse, we studied a system of long-term in vivo passages of this primary tumor for cell morphological changes, and alterations in the potential for spontaneous lung metastases. Transplants from the primary after the 4th, 20th, 40th and 80th i.m. passage (referred to as T4, T20, T40, and T80 respectively) together with their lung metastases were investigated by light microscopy, immunohistochemistry, and electron microscopy. In addition, the potential for metastasis to the lungs in each group was determined and compared with that of the parent T4 tumors. T4 tumors were mainly composed of spindle-shaped tumor cells with the ultrastructural features of fibroblasts and myofibroblasts, often arranged in a storiform or fasciculated growth pattern, and intermingled with tumor giant cells. Some small areas contained polygonal or rounded tumor cells, ultrastructurally undifferentiated, and sometimes arranged in a hemangiopericytoma-like growth pattern. Although electron-microscopical findings clearly demonstrated the mesenchymal origin of these tumor cells, immunostaining with a polyclonal antibody to vimentin was unspecific in all tumor cells and normal mouse tissue. Monoclonal antibodies to vimentin from different sources were completely negative in tumor cells and murine stromal components. In contrast, myofibroblast-like tumor cells showed immunohistochemically, a moderate to strong co-expression with monoclonal antibodies to desmin, muscle actin and α-smooth muscle actin. On the basis of these morphological findings, the primary ER 15-P was classified as a pleomorphic myofibrosarcoma. The lung metastases of T4 tumors were mainly composed of undifferentiated round to polygonal tumor cells, while the number of desmin-positive, muscle- and α-smooth muscle-actin-positive cells was reduced. The morphological features of T20 tumors and their lung metastases were the same as in T4, indicating a relative stability of the phenotype up to that stage. In contrast, T40 and T80 tumors and their lung metastases were found to contain almost exclusively undifferentiated tumor cells and many tumor giant cells. While fibroblast-like tumor cells were seen only occasionally, myofibroblast-like tumor cells had almost completely disappeared. The potential for lung metastases was nearly constant in all groups, suggesting metastatic stability. Obviously, the undifferentiated tumor cells of this model are associated with a higher metastatic potential.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01294439

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6

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Osteofibrous dysplasia of long bones — a reactive pocess to adamantinomatous tissue (1992)

Ueda, Y. ; Blasius, S. ; Edel, G. ; [et al.]

Springer

Journal of cancer research and clinical oncology 118 (1992), S. 400-400

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ISSN: 1432-1335

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01294448

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7

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Diagnose, Differentialdiagnose und Management fetaler Ovarialcysten — Erfahrungen bei 9 Fällen (1989)

Holzgreve, W. ; Edel, G. ; Gerlach, B. ; [et al.]

Springer

Archives of gynecology and obstetrics 245 (1989), S. 135-138

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ISSN: 1432-0711

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF02417213

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8

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Chondroblastoma of bone (1992)

Edel, G. ; Ueda, Y. ; Nakanishi, J. ; [et al.]

Springer

Virchows Archiv 421 (1992), S. 355-366

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ISSN: 1432-2307

Keywords: Chondroblastoma ; Bone tumours ; Immunohistochemistry

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The clinical and morphological findings of 53 chondroblastomas in the files of the Bone Tumour Registry of Westphalia are presented. The mean age of all patients was 19.2 years. The male-to-female ratio was 1.5∶1. Forty-two of the tumours (79.8%) were located in the long tubular bones and short tubular bones of the hands and were closely related to the growth plate. Six cases (11.3%) were found in the flat bones, 4 cases (7.5%) in the tarsal bones and 1 case (1.9%) in the craniofacial bones. The characteristic radiological feature of 44 investigated lesions was a mostly eccentric radiolucency with a geographic pattern of bone destruction and matrix calcifications. Periosteal reaction was evident in 9% of the cases. Most tumours demonstrate the typical morphological features of chondroblastoma, but 3 cases resembled a giant cell tumour. In 2 cases a haemangio-pericytomalike growth pattern was observed. Nine of the tumours had an aneurysmal bone cyst-like component. Vascular invasion was seen in 1 case. Immunohistochemically most cells in 30 of the cases and fetal chondroblasts in 3 cases were strongly positive with vimentin and S-100 protein. Collagen type II was positive in the chondroid matrix of the tumours and in fetal cartilage tissue; collagen type VI was present focally around individual tumour cells and was always seen in the chondroid matrix of the lesions and in fetal cartilage. These findings support the cartilaginous nature of these tumours. In paraffin sections, 46.6% of the cases revealed a distinct positive reaction of some tumour cells with the monoclonal cytokeratin antibody KL1 (molecular weight 55–57 kDa). Only 4 of them demonstrated a coexpression with the other monoclonal cytokeratin anti-body CK (clone MNF 116, molecular weight 45–56.5 kDa). In paraffin sections all fetal chondroblasts were negative with both cytokeratin antibodies. Frozen sections of 3 tumours showed a strong positive reaction with both cytokeratin antibodies in many chondroblasts, indicating an “aberrant” cytokeratin expression. Osteoclast-like giant cells stained positive with leucocyte-common antigen (LCA) and with the macrophage-associated antibody KP1, but were negative with the other macrophage-associated antibody MAC 387. Recurrence rate was 10.7%. The clinical course of all tumours was benign.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01660984

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9

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Mechanism of liver-specific metastatic tumor spread in a murine tumor model (1988)

Edel, G.

Springer

Journal of cancer research and clinical oncology 114 (1988), S. 47-58

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ISSN: 1432-1335

Keywords: Organ preference of metastases ; MCA-induced murine myofibrosarcoma ; Tumor model ER 15-P

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Malignant tumors frequently show an organ-specific metastatic spread, the causes of which are still largely unknown. Using an experimental tumor model, a methylcholanthrene-induced pleomorphic myofibrosarcoma ER 15-P of the C57 Bl6J mouse, we wanted to find out whether this phenomenon is due to an adaptation or to a selction of tumor cells. After i.v. injection of tumor cells from the primary ER 15-P into the tail vein of male mice, metastases were regularly found in the lungs, mediastinal lymph nodes, and brain, as well as in the liver and kidneys, and occasionally in the adrenals. The following experimental procedures were used to isolate a tumor cell line with a possible liver preference: (1) Tumor cells from the primary ER 15-P were injected into a mesenteric vein of male mice. Tumor cells from the resulting liver colonies were again injected into the portal system of one group of mice. In a second group, part of the same cell suspension was injected into the tail vein. This procedure was performed four times. (2) Tumor cells from the primary ER 15-P were applied into the tail vein of male mice. Tumor cells from the resulting liver metastases were reinjected directly into the tail vein. This experiment was repeated three times. (3) Tumor cells from the primary ER 15-P were injected into the tail vein of male mice. Tumor cells from liver metastases were then injected, first, into the portal system of one group of male mice, and thereafter into the tail vein of another group of animals. This experiment was repeated twice. The following results were obtained: (1) By a repeated adaptation of tumor cells from the primary ER 15-P to liver tissue, no tumor cell line could be isolated that would show a preferential metastic spread to this organ after tail-vein injection. (2) Repeated i.v. passages of tumor cells from liver metastases into the tail vein led to the selection of a tumor cell line with a tendency to liver metastasis. (3) Tumor cells selected from liver metastases induced via tailvein injection showed, after a prolonged stay in the liver and a successive i.v. passage into the tail vein, a marked specificity for this organ. These results indicate that the liver-specific spread of tumor cells in our model is based on the selection of a tumor cell line from the primary ER 15-P influenced by the hepatic microenvironment.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00390485

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Osteofibrous dysplasia of long bones—a reactive process to adamantinomatous tissue (1992)

Ueda, Y. ; Blasius, S. ; Edel, G. ; [et al.]

Springer

Journal of cancer research and clinical oncology 118 (1992), S. 152-156

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ISSN: 1432-1335

Keywords: Osteofibrous dysplasia ; Adamantinoma ; Cytokeratin ; Immunohistochemistry

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The most controversial aspect of osteofibrous dysplasia (OFD) is its possible histogenetic relationship to adamantinoma of long bone. Evidence is recently beginning to accumulate that OFD may be a reactive process to regressive adamantinoma. To verify the concept, 13 lesions of OFD were studied again by immunohistochemistry for cytokeratins of different molecular masses, as well as by conventional stainings. In addition, 2 adamantinomas and 6 fibrous dysplasias of the tibia were studied for reference. A small number of spindle- or ovoid-shaped cells scattered individually in the fibro-osseous stroma showed positive reactions for cytokeratins of 55–57 kDa in 2 lesions, and for those of 45–56.5 kDa in 8 lesions of 13 OFDs, although no definite epithelial island could be detected even by immunohistochemistry. Adamantinomas also showed single cytokeratin-positive cells dispersed in fibroblastic stroma, in addition to epithelial islands positive for cytokeratins of both 55–57 kDa and 45–56,5 kDa. All cases of fibrous dysplasia were negative for cytokeratins. During the observation, no case of OFDs progressed to classic adamantinoma. The present study, demonstrating the existence of an intermediate stage between “differentiated adamantinoma” and total elimination of adamantinomatous components, gives further support for the concept that OFD is a secondary reactive process to adamantinomatous tissue. In practice, the existence of single scattered cytokeratin-immunoreactive cells in otherwise typical OFDs may not indicate the truly malignant behaviour of classic adamantinoma, unless discrete epithelioid cell nests are also found.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01187505

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